Zuliani-Alvarez Lorena, Midwood Kim S
Nuffield Department of Orthopaedics, Rheumatology and Musculoskeletal Sciences, Kennedy Institute of Rheumatology, University of Oxford , Oxford, United Kingdom .
Adv Wound Care (New Rochelle). 2015 May 1;4(5):273-285. doi: 10.1089/wound.2014.0599.
Fibrinogen-related proteins (FRePs) comprise an intriguing collection of extracellular molecules, each containing a conserved fibrinogen-like globe (FBG). This group includes the eponymous fibrinogen as well as the tenascin, angiopoietin, and ficolin families. Many of these proteins are upregulated during tissue repair and exhibit diverse roles during wound healing. An increasing body of evidence highlights the specific expression of a number of FRePs following tissue injury and infection. Upon induction, each FReP uses its FBG domain to mediate quite distinct effects that contribute to different stages of tissue repair, such as driving coagulation, pathogen detection, inflammation, angiogenesis, and tissue remodeling. Despite a high degree of homology among FRePs, each contains unique sequences that enable their diversification of function. Comparative analysis of the structure and function of FRePs and precise mapping of regions that interact with a variety of ligands has started to reveal the underlying molecular mechanisms by which these proteins play very different roles using their common domain. Fibrinogen has long been used in the clinic as a synthetic matrix serving as a scaffold or a delivery system to aid tissue repair. Novel therapeutic strategies are now emerging that harness the use of other FRePs to improve wound healing outcomes. As we learn more about the underlying mechanisms by which each FReP contributes to the repair response, specific blockade, or indeed potentiation, of their function offers real potential to enable regulation of distinct processes during pathological wound healing.
纤维蛋白原相关蛋白(FRePs)是一类引人关注的细胞外分子集合,每个分子都含有一个保守的纤维蛋白原样结构域(FBG)。该组包括同名的纤维蛋白原以及腱生蛋白、血管生成素和纤维胶凝蛋白家族。这些蛋白中的许多在组织修复过程中上调,并在伤口愈合过程中发挥多种作用。越来越多的证据突出了多种FRePs在组织损伤和感染后的特异性表达。诱导后,每种FReP利用其FBG结构域介导截然不同的效应,这些效应有助于组织修复的不同阶段,如促进凝血、病原体检测、炎症、血管生成和组织重塑。尽管FRePs之间具有高度同源性,但每个都包含独特的序列,使其功能多样化。对FRePs的结构和功能进行比较分析以及与各种配体相互作用区域的精确映射,已开始揭示这些蛋白利用其共同结构域发挥非常不同作用的潜在分子机制。纤维蛋白原长期以来在临床上被用作合成基质,作为支架或递送系统来辅助组织修复。现在正在出现新的治疗策略,利用其他FRePs来改善伤口愈合结果。随着我们更多地了解每种FReP对修复反应的潜在机制,对其功能的特异性阻断或增强确实提供了在病理性伤口愈合过程中调节不同过程的真正潜力。